Study of Renal Accumulation of Targeted Polycations in Acute Kidney Injury

Tang, Weimin; Panja, Subhash Chandra; Jogdeo, Chinmay M.; Tang, Siyuan; Yu, Ao; Oupický, David

doi:10.1021/acs.biomac.2c00079

Cited by 3 publications

(3 citation statements)

References 48 publications

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“…Nanotechnology-based drug delivery systems have facilitated AKI therapy, such as early prevention, early diagnosis, drug delivery, and gene therapy. − In particular, stimulus-responsive polymeric drug delivery systems have attracted increasing attention for low toxicity, less side effects, prone accumulation into targeted tissues, and response to the disease microenvironment. − Liu et al synthesized a ROS-responsive prodrug based on chitosan-SS31 for AKI therapy. The prodrug presented ROS-responsive drug release leading to an enhanced therapeutic effect of SS31.…”

Section: Introductionmentioning

confidence: 99%

Dual-Responsive Curcumin-Loaded Nanoparticles for the Treatment of Cisplatin-Induced Acute Kidney Injury

et al. 2022

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Acute kidney injury (AKI) has been a global public health concern leading to high patient morbidity and mortality in the world. Nanotechnology-mediated antioxidative therapy has facilitated the treatment of AKI. Herein, a hierarchical curcumin-loaded nanodrug delivery system (NPS@Cur) was fabricated for antioxidant therapy to ameliorate AKI. The nanoplatform could respond to subacidic and reactive oxygen species (ROS) microenvironments. The subacidic microenvironment led to a smaller size (from 140.9 to 99.36 nm) and positive charge (from −4.9 to 12.6 mV), contributing to the high accumulation of nanoparticles. An excessive ROS microenvironment led to nanoparticle degradation and drug release. In vitro assays showed that NPS@Cur could scavenge excessive ROS and relieve oxidative stress in H2O2-induced HK-2 cells through reduced apoptosis, activated autophagy, and decreased endoplasmic reticulum stress. Results from cisplatin-induced AKI models revealed that NPS@Cur could effectively alleviate mitochondria injury and protect kidneys via antioxidative protection, activated autophagy, decreased endoplasmic reticulum stress, and reduced apoptosis. NPS@Cur showed excellent biocompatibility and low toxicity to primary tissues in mice. These results revealed that NPS@Cur may be a potential therapeutic strategy for efficiently treating cisplatin or other cause-induced AKI.

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Section: Introductionmentioning

confidence: 99%

Dual-Responsive Curcumin-Loaded Nanoparticles for the Treatment of Cisplatin-Induced Acute Kidney Injury

et al. 2022

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“…AFB1 generally requires metabolic activation to the 8,9-epoxide to produce toxicity by DNA and protein adducts [38] making liver a primary target organ, although AFB1 adducts have also been documented in the kidneys of rats and mice [39]. Here, only the LgT moRPTECs showed substantial transcriptional changes (1139 DEGs) in response to AFB1 at 72 h. Upregulation of typical toxicity markers like Kim1 (Havcr1), Il6, and Mmp's were observed with only minor increases in the LgT cells after 72 h. However, AFB1-mediated increases by concentration for Cxcr4 [40,41] and Il6 [42] are consistent markers of kidney injury. Such changes could be responsible for the induction of multiple developmental transcription factors [43,44] such as Barx1, Gbx2, Nkx2-9, Tlx3, Tfap2e, and Hoxc12.…”

Section: Discussionmentioning

confidence: 84%

Insights into Repeated Renal Injury Using RNA-Seq with Two New RPTEC Cell Lines

Merrick,

Martin,

Brooks

et al. 2023

IJMS

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Renal proximal tubule epithelial cells (RPTECs) are a primary site for kidney injury. We created two RPTEC lines from CD-1 mice immortalized with hTERT (human telomerase reverse transcriptase) or SV40 LgT antigen (Simian Virus 40 Large T antigen). Our hypothesis was that low-level, repeated exposure to subcytotoxic levels of 0.25–2.5 μM cisplatin (CisPt) or 12.5–100 μM aflatoxin B1 (AFB1) would activate distinctive genes and pathways in these two differently immortalized cell lines. RNA-seq showed only LgT cells responded to AFB1 with 1139 differentially expressed genes (DEGs) at 72 h. The data suggested that AFB1 had direct nephrotoxic properties on the LgT cells. However, both the cell lines responded to 2.5 μM CisPt from 3 to 96 h expressing 2000–5000 total DEGs. For CisPt, the findings indicated a coordinated transcriptional program of injury signals and repair from the expression of immune receptors with cytokine and chemokine secretion for leukocyte recruitment; robust expression of synaptic and substrate adhesion molecules (SAMs) facilitating the expression of neural and hormonal receptors, ion channels/transporters, and trophic factors; and the expression of nephrogenesis transcription factors. Pathway analysis supported the concept of a renal repair transcriptome. In summary, these cell lines provide in vitro models for the improved understanding of repeated renal injury and repair mechanisms. High-throughput screening against toxicant libraries should provide a wider perspective of their capabilities in nephrotoxicity.

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“…Small interfering RNA (siRNA) nanocarriers that also transported CXCR4 antagonists (CXCR4a) successfully reduced inflammation and AKI [31 ▪ ,32 ▪ ]. Surface chemistry optimization of CXCR4a nanoparticles, leads to better kidney targeting [33 ▪ ]. Cell-free DNA (cfDNA) is abundant during AKI and is considered to increase local inflammation.…”

Section: Acute Kidney Injurymentioning

confidence: 99%

Nanomedicine in kidney disease

Bishop

Sharma

Scott

2023

Current Opinion in Nephrology &Amp; Hypertension

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Purpose of reviewThe pathophysiological understanding of kidney-related disorders has profoundly increased; however, tissuespecific and cell-specific treatments in this field remain scarce. Advances in nanomedicine enable alteration of pharmacokinetics and targeted treatments improving efficiency and reducing toxicity. This review addresses recent developments of nanocarriers used for various purposes in the broad field of kidney disease, which may pave a path to new therapeutic and diagnostic solutions employing nanomedicine. Recent findingsControlled delivery of antiproliferative medications enables improved treatment of polycystic kidney disease and fibrosis. Directed anti-inflammatory treatment mitigated glomerulonephritis and tubulointerstitial nephritis. Multiple injury pathways in AKI have been targeted, with therapeutic solutions for oxidative stress, mitochondrial dysfunction, local inflammation and improving self-repair mechanisms. In addition to such treatment development, noninvasive early detection methods (minutes after ischemic insult) have been demonstrated as well. Sustained release of therapies that reduce ischemia--reperfusion injury as well as new aspects for immunosuppression bring hope to improving kidney transplant outcomes. The latest breakthroughs in gene therapy are made achievable by engineering the targeted delivery of nucleic acids for new treatments of kidney disease. SummaryRecent advances in nanotechnology and pathophysiological understanding of kidney diseases show potential for translatable therapeutic and diagnostic interventions in multiple etiologies of kidney disease.

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Study of Renal Accumulation of Targeted Polycations in Acute Kidney Injury

Cited by 3 publications

References 48 publications

Dual-Responsive Curcumin-Loaded Nanoparticles for the Treatment of Cisplatin-Induced Acute Kidney Injury

Dual-Responsive Curcumin-Loaded Nanoparticles for the Treatment of Cisplatin-Induced Acute Kidney Injury

Insights into Repeated Renal Injury Using RNA-Seq with Two New RPTEC Cell Lines

Nanomedicine in kidney disease

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